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BriX: a database of protein building blocks for structural analysis, modeling and design

机译:BriX:用于结构分析,建模和设计的蛋白质构件的数据库

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High-resolution structures of proteins remain the most valuable source for understanding their function in the cell and provide leads for drug design. Since the availability of sufficient protein structures to tackle complex problems such as modeling backbone moves or docking remains a problem, alternative approaches using small, recurrent protein fragments have been employed. Here we present two databases that provide a vast resource for implementing such fragment-based strategies. The BriX database contains fragments from over 7000 non-homologous proteins from the Astral collection, segmented in lengths from 4 to 14 residues and clustered according to structural similarity, summing up to a content of 2 million fragments per length. To overcome the lack of loops classified in BriX, we constructed the Loop BriX database of non-regular structure elements, clustered according to end-to-end distance between the regular residues flanking the loop. Both databases are available online (http://brix.crg.es) and can be accessed through a user-friendly web-interface. For high-throughput queries a web-based API is provided, as well as full database downloads. In addition, two exciting applications are provided as online services: (i) user-submitted structures can be covered on the fly with BriX classes, representing putative structural variation throughout the protein and (ii) gaps or low-confidence regions in these structures can be bridged with matching fragments.
机译:蛋白质的高分辨率结构仍然是了解其在细胞中功能的最有价值的来源,并为药物设计提供了线索。由于有足够的蛋白质结构来解决复杂的问题,例如对骨架移动或对接建模,仍然是一个问题,因此已采用了使用小型重复蛋白质片段的替代方法。在这里,我们介绍了两个数据库,它们为实施此类基于片段的策略提供了大量资源。 BriX数据库包含来自Astral集合的7000多种非同源蛋白质的片段,其长度从4个残基切成14个残基,并根据结构相似性进行聚类,每长度总和为200万个片段。为了克服在BriX中分类的循环的不足,我们构建了非规则结构元素的Loop BriX数据库,并根据位于循环两侧的常规残基之间的端到端距离进行聚类。这两个数据库都可以在线获得(http://brix.crg.es),并且可以通过用户友好的Web界面进行访问。对于高通量查询,提供了基于Web的API,以及完整的数据库下载。此外,在线服务还提供了两个激动人心的应用程序:(i)BriX类可以即时覆盖用户提交的结构,代表整个蛋白质的假定结构变化;(ii)这些结构中的缺口或低信度区域可以与匹配的片段桥接。

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